MEDFORD/SOMERVILLE, Mass. (May 26, 2019)-- Researchers led by biologists at Tufts University have discovered that the brains of developing frog embryos damaged by nicotine exposure can be repaired by treatment with certain drugs called "ionoceuticals" that drive the recovery of bioelectric patterns in the embryo, followed by repair of normal anatomy, gene expression and brain function in the growing tadpole. The research, published today in Frontiers in Neuroscience, introduces intervention strategies based on restoring the bioelectric "blueprint" for embryonic development, which the researchers suggest could provide a roadmap for the exploration of therapeutic drugs to help repair birth defects.
Earlier studies had shown that nicotine disrupts the normal electrical patterns in the brain of the growing embryo, basically washing out, or reducing the contrast, of the bioelectric blueprint -- a "map" of varying voltage levels around the cells that guides the pattern and growth of tissues and organs. Nicotine in humans has been linked to prenatal morbidity, sudden infant death, attention deficit hypersensitivity disorder (ADHD), and other deficits in cognitive function, learning, and memory, but many questions had remained about how this molecule induces structural defects in the brain.
The authors applied nicotine to developing frog embryos to create neural defects with the intention of identifying specific interventions that could reverse the chemical's harmful effects. Their previous research identified one particular element in the natural electric signalling that controls brain development, hyperpolarization-activated cyclic nucleotide gated channel-2 (HCN2), which was able to restore the bioelectric patterns - much like dialing up the contrast with a photo edit tool - and protect against nicotine-induced defects.
There are two major new discoveries in this study. First, unlike the prior work in which a form of gene therapy modifying the expression of HCN2 was used to repair the defects, the new experiments showed that the same effect can be achieved without introducing a gene - instead, small molecule drugs were used to activate HCN2 channels already present in the frog embryo. Second, the researchers demonstrated that the electrical patterning information that governs brain development can be reset from a distant location on the embryo.
"What was remarkable about the experiments in this study is that when we increased expression of HCN2 at a distance from the brain, in non-neural regions, the defects in the brain were still repaired or prevented," said Michael Levin, Vannevar Bush Professor of Biology at Tufts University's School of Arts and Sciences and director of the Allen Discovery Center at Tufts. "We saw that HCN2 in one part of the embryo could restore the bioelectric pattern not only locally, but at a distance as well."
"The instructions to build a fully grown animal, including organs as complex as the brain, are distributed among all the cells of the embryo," he added. "These results suggest that we might not have to directly target the damaged region, and we can use drugs instead of genetic manipulation, which opens a lot of opportunities for biomedical deployment."
In a developing embryo, the bioelectric signals help guide the patterning of tissue and organ formation, as well as regeneration after injury. They are formed by electrically charged ions moving in and out of cells to create voltage differences across the cell membranes. The pattern of voltage differences among the entire ensemble of cells in the embryo helps guide asymmetry between left and right sides of the body, the formation and development of heart, muscle, limbs and face, and of course the growth and organization of the most complex organ in the body - the brain.
A computational model of an ensemble of cells representing an embryo and its electrical patterns confirmed that rescuing normal brain development from nicotine damage did not require specific targeting of the damaged region. HCN2 increases the hyperpolarization of a cell (increased internal negative charges), so when the model was asked to hyperpolarize a small patch of tissue far from the brain, that patch could propagate and restore polarization of regions all the way to the brain, setting the stage for normal development.
"When thinking about birth defects, especially involving the brain, these results suggest that we don't need to target the specific region that is damaged. We can place the fix almost anywhere in the embryo, and the information will communicate with the rest of the embryo to reset the body's instructions back to normal," said Vaibhav Pai, Ph.D., research scientist at the Allen Discovery Center at Tufts and first author of the study. "That led us to think, could we find a drug that activated HCN2, and use that to prevent defects anywhere in the embryo, or even repair defects that are already underway?"
Drugs that activate HCN2 exist - lamotrigine and gabapentin - and they are already FDA approved for other indications. The researchers again exposed the frog embryos to nicotine, and then treated them with the drugs at different stages of embryonic development. Nicotine-exposed embryos that were not treated with drugs led to about 68% of tadpoles with brain defects. By comparison, treatment of nicotine exposed embryos with lamotrigine or gabapentin led to significant reduction in brain defects (as few as 10% and 16% of tadpoles with brain defects, respectively).
Restoration extended beyond electrical and physically observed defects, as the authors demonstrated that nicotine-exposed tadpoles treated with the drugs not only restored expression of genetic markers of normal brain development, but remarkably, exhibited normal learning capacity (e.g. training to avoid red light), which is lost in untreated nicotine-exposed tadpoles, showing a very complete rescue from molecular histology to behavior.
Other authors of this study include: Javier Cervera, Profesor, associate professor of the Unversity of Valencia, Spain; Valerie Willocq and Emma Lederer, research assistants in the Levin lab at the Allen Discovery Center at Tufts.
This research was supported by the Paul G. Allen Frontiers Group (12171), G. Harold and Leila Y. Mathers Charitable Foundation (TFU141), the Templeton World Charity Foundation (TWCF0089/AB55), the Ministerio de Ciencia, Innovación y Universidades (Spain) and the European Regional Development Funds (FEDER) (PGC2018-097359-B-I00), and the National Institutes of Health (AR055993-01, AR061988). The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health.
Pai, V., Cervera, J., Mafe, S., Willocq, V., Lederer, E., and Levin, M. "HCN2 channel-induced rescue of brain teratogenesis via local and long-range bioelectric repair" Frontiers in Neuroscience 2020 May 26; DOI: 10.3389/fncel.2020.00136
About Tufts University
Tufts University, located on campuses in Boston, Medford/Somerville and Grafton, Massachusetts, and in Talloires, France, is recognized among the premier research universities in the United States. Tufts enjoys a global reputation for academic excellence and for the preparation of students as leaders in a wide range of professions. A growing number of innovative teaching and research initiatives span all Tufts campuses, and collaboration among the faculty and students in the undergraduate, graduate and professional programs across the university's schools is widely encouraged.
Frontiers in Neuroscience